人类胚胎神经祖细胞暴露于农药的表型和生物力学特征

Marissa C. Sarsfield, Jennifer Vasu, Sabreen M. Abuoun, N. Allena, C. Kothapalli
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引用次数: 0

摘要

据报道,各种形式的杀虫剂都是对人类健康有害的环境毒物。这些制剂的活性成分可以通过空气、食物或水进入人体。流行病学研究表明,这些化合物在胎儿和婴儿阶段强烈影响发育中的大脑,因为它们能够突破发育不全的血脑屏障。由于发育中的大脑中的神经祖细胞最容易受到这些化合物的影响,因此必须研究神经祖细胞在接触这些化学物质时产生毒性的机制。在这里,我们使用Live/Dead®和Hoechst染色评估了在六种广泛使用的杀虫剂的活性成分存在的情况下,人类胎儿NPC在2D培养物中的生存能力。IC50值范围为4.1–201μM。随着毒物浓度的增加,细胞活力显著下降(p<0.01),毒性顺序为马拉硫磷<4-氨基吡啶<甲氧苄啶<丙烯菊酯<特马福思本文章由计算机程序翻译,如有差异,请以英文原文为准。
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Phenotypic and Biomechanical Characteristics of Human Fetal Neural Progenitor Cells Exposed to Pesticide Compounds
Various forms of pesticides have been reported to be among the environmental toxicants, which are detrimental to human health. The active ingredients of these formulations can enter the human body through air, food, or water. Epidemiological studies suggest that these compounds strongly affect the developing brain in fetal and infant stages due to their ability to breach the underdeveloped blood–brain barrier. Since neural progenitor stem cells (NPCs) in the developing brain are the most vulnerable to these compounds, the mechanisms by which NPCs experience toxicity upon exposure to these chemicals must be investigated. Here, we assessed the viability of human fetal NPCs in 2D cultures in the presence of the active ingredients of six widely used pesticides using Live/Dead® and Hoechst staining. The IC50 values ranged from 4.1–201 μM. A significant drop in cell viability with increasing toxicant concentration (p < 0.01) was noted, with the order of toxicity being malathion < 4-aminopyridine < methoprene < prallethrin < temephos < pyriproxyfen. Changes in cellular biomechanical characteristics (Young’s modulus, tether force, membrane tension, and tether radius) were quantified using atomic force microscopy, whereas cell migration was elucidated over 48 h using a customized wound-healing assay. The Young’s modulus of fetal NPCs exposed to IC50/2 doses of these compounds was reduced by 38–70% and that of those exposed to IC50 doses was reduced by 71–80% (p < 0.001 vs. controls for both; p < 0.01 for IC50 vs. IC50/2 for each compound). Similar patterns were noted for tether forces and membrane tension in fetal NPCs. NPC migration was found to be compound type- and dose-dependent. These results attest to the significant detrimental effects of these compounds on various aspects of the human fetal NPC phenotype, and the utility of cell mechanics as a marker to assess developmental neurotoxicity.
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Biophysica
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1.60
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